Vitamin A is required for formation of most organs and tissues including the kidney. Our studies demonstrate the requirement for 2 vitamin A receptors Rara and Rarb2 and Raldh2, a RA-synthesizing enzyme in stromal mesenchyme for normal renal development. In cortical stromal cells, Rara and Rarb2 are likely to be important for growth and branching of the renal collecting system, controlling expression of Ret at branching collecting duct tips where Ret is essential for branching morphogenesis. Definitive proof of this hypothesis is dependent on identification of vitamin A-inducible stromal factors that modulate Ret expression. We will identify these factors using differential hybridization and microarray analysis. Recent studies revealed medullary abnormalities in Rarab2- and Raldh2- mice at El8, suggesting a possible role for vitamin A signaling during tubule extension or collecting duct morphogenesis in the medulla. Consistent with this suggestion, we fmd a novel domain of RA synthesis in the immature loop of Henle, specifically in the hairpin turn, the site of tubule elongation, and we find that Rara and Rarb2 are co-localized in medullary stromal cells surrounding the large collecting ducts and loops of Henle, suggesting that vitamin A signaling in medullary stroma controls late stages of tubule elongation, collecting duct morphogenesis, or both. Alternately, impaired Vitamin A signaling at early stages may be the cause of medullary abnormalities. We will distinguish between these possibilities by generating mutants in which stromal cell signaling can be inducibly inactivated using the Tet-on system, then we will test the requirement for vitamin A in stromal cells at early and late stages. A new RA-synthesizing enzyme, Raldh3, has recently been identified. Raldh3 is localized exclusively in the ureteric bud and compound mutants lacking both Raldh2 and Raldh3 display more severe renal phenotypes than single Raldh2 or Raldh2 mutants, suggesting that RA-synthesis in the ureteric bud may be important directly, or indirectly activating vitamin A signaling in stromal cells. We will distinguish between these possibilities by generating mouse mutants in which the RA-response has been blocked either in the ureteric bud or in stroma by expression of a dominant negative Rar protein.

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
5P01DK055388-08
Application #
7188668
Study Section
Special Emphasis Panel (ZDK1)
Project Start
Project End
Budget Start
2006-01-01
Budget End
2006-12-31
Support Year
8
Fiscal Year
2006
Total Cost
$358,431
Indirect Cost
Name
Columbia University (N.Y.)
Department
Type
DUNS #
621889815
City
New York
State
NY
Country
United States
Zip Code
10032
Correnti, Colin; Richardson, Vera; Sia, Allyson K et al. (2012) Siderocalin/Lcn2/NGAL/24p3 does not drive apoptosis through gentisic acid mediated iron withdrawal in hematopoietic cell lines. PLoS One 7:e43696
Oliver, Juan A; Maarouf, Omar; Cheema, Faisal H et al. (2012) SDF-1 activates papillary label-retaining cells during kidney repair from injury. Am J Physiol Renal Physiol 302:F1362-73
Batourina, Ekaterina; Gandhi, Devangini; Mendelsohn, Cathy L et al. (2012) Organotypic culture of the urogenital tract. Methods Mol Biol 886:45-53
Paragas, Neal; Qiu, Andong; Zhang, Qingyin et al. (2011) The Ngal reporter mouse detects the response of the kidney to injury in real time. Nat Med 17:216-22
Costantini, Frank; Watanabe, Tomoko; Lu, Benson et al. (2011) Dissection of embryonic mouse kidney, culture in vitro, and imaging of the developing organ. Cold Spring Harb Protoc 2011:pdb.prot5613
Sola-Del Valle, David A; Mohan, Sumit; Cheng, Jen-Tse et al. (2011) Urinary NGAL is a useful clinical biomarker of HIV-associated nephropathy. Nephrol Dial Transplant 26:2387-90
Bao, Guanhu; Clifton, Matthew; Hoette, Trisha M et al. (2010) Iron traffics in circulation bound to a siderocalin (Ngal)-catechol complex. Nat Chem Biol 6:602-9
Michos, Odyssé; Cebrian, Cristina; Hyink, Deborah et al. (2010) Kidney development in the absence of Gdnf and Spry1 requires Fgf10. PLoS Genet 6:e1000809
Costantini, Frank (2010) GDNF/Ret signaling and renal branching morphogenesis: From mesenchymal signals to epithelial cell behaviors. Organogenesis 6:252-62
Parravicini, Elvira; Nemerofsky, Sheri L; Michelson, Kenneth A et al. (2010) Urinary neutrophil gelatinase-associated lipocalin is a promising biomarker for late onset culture-positive sepsis in very low birth weight infants. Pediatr Res 67:636-40

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